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Malaria Journal
Published in: Malaria Journal 1/2009

Open Access 01-12-2009 | Methodology

Towards optimal design of anti-malarial pharmacokinetic studies

Authors: Julie A Simpson, Kris M Jamsen, Ric N Price, Nicholas J White, Niklas Lindegardh, Joel Tarning, Stephen B Duffull

Published in: Malaria Journal | Issue 1/2009

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Abstract

Background

Characterization of anti-malarial drug concentration profiles is necessary to optimize dosing, and thereby optimize cure rates and reduce both toxicity and the emergence of resistance. Population pharmacokinetic studies determine the drug concentration time profiles in the target patient populations, including children who have limited sampling options. Currently, population pharmacokinetic studies of anti-malarial drugs are designed based on logistical, financial and ethical constraints, and prior knowledge of the drug concentration time profile. Although these factors are important, the proposed design may be unable to determine the desired pharmacokinetic profile because there was no formal consideration of the complex statistical models used to analyse the drug concentration data.

Methods

Optimal design methods incorporate prior knowledge of the pharmacokinetic profile of the drug, the statistical methods used to analyse data from population pharmacokinetic studies, and also the practical constraints of sampling the patient population. The methods determine the statistical efficiency of the design by evaluating the information of the candidate study design prior to the pharmacokinetic study being conducted.

Results

In a hypothetical population pharmacokinetic study of intravenous artesunate, where the number of patients and blood samples to be assayed was constrained to be 50 and 200 respectively, an evaluation of varying elementary designs using optimal design methods found that the designs with more patients and less samples per patient improved the precision of the pharmacokinetic parameters and inter-patient variability, and the overall statistical efficiency by at least 50%.

Conclusion

Optimal design methods ensure that the proposed study designs for population pharmacokinetic studies are robust and efficient. It is unethical to continue conducting population pharmacokinetic studies when the sampling schedule may be insufficient to estimate precisely the pharmacokinetic profile.
Appendix
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Metadata
Title
Towards optimal design of anti-malarial pharmacokinetic studies
Authors
Julie A Simpson
Kris M Jamsen
Ric N Price
Nicholas J White
Niklas Lindegardh
Joel Tarning
Stephen B Duffull
Publication date
01-12-2009
Publisher
BioMed Central
Published in
Malaria Journal / Issue 1/2009
Electronic ISSN: 1475-2875
DOI
https://doi.org/10.1186/1475-2875-8-189

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